细胞膜与细胞核之间的通讯:蛋白质区隔化的作用。

S A Lelièvre, M J Bissell
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引用次数: 0

摘要

了解信息是如何从细胞外传递到细胞内的是所有参与信号转导的生物学家面临的一个关键挑战。由细胞-细胞和细胞-细胞外基质接触引发的信息流是由涉及多种蛋白质的粘附复合物的形成介导的。在黏附复合物内部,结缔膜骨架蛋白(CMS)是与黏附分子结合、组织细胞骨架并启动生化级联反应的信号转导。粘附复合物介导的信号转导最终指导细胞核中超分子结构的形成,如dna结合转录因子的多个复合物的建立,以及核结构蛋白的重新分配形成核亚结构域。最近,一些CMS蛋白被观察到可以进入细胞核,这表明这些蛋白在信号转导中起着独特的作用。本文综述了膜骨架结构信号转导的核易位,并扩展了我们对驻留核蛋白在膜骨架上可能易位的分析。这使我们设想空间上遥远的细胞区室(即膜骨架和细胞核)之间的通信是基于微妙的多层次结构和生化平衡的双向信息流(动态互惠)。在一个层面上,它是由结构信号转导及其结合伙伴之间的相互作用介导的,在另一个层面上,它可能是由不同细胞室中信号转导的平衡和整合介导的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Communication between the cell membrane and the nucleus: role of protein compartmentalization.

Understanding how the information is conveyed from outside to inside the cell is a critical challenge for all biologists involved in signal transduction. The flow of information initiated by cell-cell and cell-extracellular matrix contacts is mediated by the formation of adhesion complexes involving multiple proteins. Inside adhesion complexes, connective membrane skeleton (CMS) proteins are signal transducers that bind to adhesion molecules, organize the cytoskeleton, and initiate biochemical cascades. Adhesion complex-mediated signal transduction ultimately directs the formation of supramolecular structures in the cell nucleus, as illustrated by the establishment of multi complexes of DNA-bound transcription factors, and the redistribution of nuclear structural proteins to form nuclear subdomains. Recently, several CMS proteins have been observed to travel to the cell nucleus, suggesting a distinctive role for these proteins in signal transduction. This review focuses on the nuclear translocation of structural signal transducers of the membrane skeleton and also extends our analysis to possible translocation of resident nuclear proteins to the membrane skeleton. This leads us to envision the communication between spatially distant cellular compartments (i.e., membrane skeleton and cell nucleus) as a bidirectional flow of information (a dynamic reciprocity) based on subtle multilevel structural and biochemical equilibria. At one level, it is mediated by the interaction between structural signal transducers and their binding partners, at another level it may be mediated by the balance and integration of signal transducers in different cellular compartments.

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